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Peer-reviewed veterinary case report

New blood test to check bleeding problems in dogs

By Tomoko Iwanaga et al.·Published in Frontiers in Veterinary Science·2020·Joint Faculty of Veterinary Medicine, Kagoshima University, Kagoshima, Japan, CH·View original on DOAJ

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Original publication title: A Novel Microchip Flow Chamber (Total Thrombus Analysis System) to Assess Canine Hemostasis

Species:
dog
Stomach & digestionDogs

Plain-English summary

A group of dogs with bleeding disorders, including von Willebrand's disease and hemophilia A, were tested using a new device called the Total-Thrombus Analysis System (T-TAS) to see how well it could assess their blood clotting ability. The T-TAS showed that these dogs had abnormal blood clotting compared to healthy dogs, which could help veterinarians better understand their bleeding risks. The device recorded how quickly and effectively blood clots formed, providing valuable information for treatment decisions. This study suggests that the T-TAS could be a useful tool for diagnosing and managing bleeding disorders in dogs.

People also search for: dog bleeding disorder treatment · von Willebrand's disease in dogs · hemophilia A symptoms in dogs

Abstract

Hemorrhagic diseases are common in dogs. Current coagulation assays do not model all aspects of in vivo hemostasis and may not predict bleeding risk. The Total-Thrombus Analysis System (T-TAS) is a novel hemostasis assay system in which whole blood flows through microfluidic channels at defined shear rates to provide qualitative and quantitative evaluation of platelet function (PL-chip) and coagulation function (AR-chip). The present study evaluated the T-TAS in dogs with hereditary bleeding disorders and with acquired hemorrhagic syndromes (Group 1), and healthy controls (Group 2). Hereditary defects included von Willebrand's disease (VWD; n = 4), hemophilia A (n = 2), and canine Scott syndrome (n = 2). Acquired hemorrhagic disorders included neoplastic hemoperitoneum (n = 2) and acute hemorrhagic diarrhea syndrome (n = 1). Citrate anticoagulated samples were collected from diseased dogs (Group 1, n = 11) and controls (Group 2, n = 11) for coagulation screening tests, fibrinogen analyses, D-dimer concentration, antithrombin activity, von Willebrand Factor antigen, PFA-100 closure time (PFA-CT), and thromboelastography (TEG). Citrate and hirudin anticoagulated samples were used for T-TAS analyses at two shear rates. Qualitative thrombus formation in each chip was recorded using the T-TAS video camera. Numeric parameters, derived from the instrument software, included occlusion start time (OST; time to 10 kPa), occlusion time (OT; time to 60 kPa (PL-chip) or 80 kPa (AR-chip)), and area under the pressure curve (AUC). Correlations between continuous variables were evaluated by Spearman's rank. Continuous variables were compared between groups by Student's t-test or the Mann-Whitney U-test. Alpha was set at 0.05. In combined analyses of all dogs, significant correlations were identified between T-TAS variables, between the PFA-CT and PL-chip parameters and between TEG variables and AR-chip parameters. The prothrombin time correlated with the AR-chip AUC at both shear rates. In Group 1 dogs, the AR-chip AUC at low shear was significantly reduced compared with Group 2 dogs. Aberrant thrombus formation was seen in video images recorded from dogs with VWD and hemophilia A. The T-TAS AR-chip analysis distinguished dogs with bleeding risk compared to healthy controls. Initial evaluations of the T-TAS suggest it may aid characterization of hemostasis in patients at-risk of bleeding and assist with delineating bleeding phenotypes.

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Original publication on DOAJ: https://doi.org/10.3389/fvets.2020.00307